Literature DB >> 25496009

The Slx4-Dpb11 scaffold complex: coordinating the response to replication fork stalling in S-phase and the subsequent mitosis.

Lissa N Princz1, Dalia Gritenaite, Boris Pfander.   

Abstract

Replication fork stalling at DNA lesions is a common problem during the process of DNA replication. One way to allow the bypass of these lesions is via specific recombination-based mechanisms that involve switching of the replication template to the sister chromatid. Inherent to these mechanisms is the formation of DNA joint molecules (JMs) between sister chromatids. Such JMs need to be disentangled before chromatid separation in mitosis and the activity of JM resolution enzymes, which is under stringent cell cycle control, is therefore up-regulated in mitosis. An additional layer of control is facilitated by scaffold proteins. In budding yeast, specifically during mitosis, Slx4 and Dpb11 form a cell cycle kinase-dependent complex with the Mus81-Mms4 structure-selective endonuclease, which allows efficient JM resolution by Mus81. Furthermore, Slx4 and Dpb11 interact even prior to joining Mus81 and respond to replication fork stalling in S-phase. This S-phase complex is involved in the regulation of the DNA damage checkpoint as well as in early steps of template switch recombination. Similar interactions and regulatory principles are found in human cells suggesting that Slx4 and Dpb11 may have an evolutionary conserved role organizing the cellular response to replication fork stalling.

Entities:  

Keywords:  DNA damage response; cell cycle; homologous recombination; joint molecule resolution; post-replicative repair

Mesh:

Substances:

Year:  2015        PMID: 25496009      PMCID: PMC4612105          DOI: 10.4161/15384101.2014.989126

Source DB:  PubMed          Journal:  Cell Cycle        ISSN: 1551-4005            Impact factor:   4.534


  43 in total

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Review 5.  Timing and spacing of ubiquitin-dependent DNA damage bypass.

Authors:  Helle D Ulrich
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6.  Human SLX4 is a Holliday junction resolvase subunit that binds multiple DNA repair/recombination endonucleases.

Authors:  Samira Fekairi; Sarah Scaglione; Charly Chahwan; Ewan R Taylor; Agnès Tissier; Stéphane Coulon; Meng-Qiu Dong; Cristian Ruse; John R Yates; Paul Russell; Robert P Fuchs; Clare H McGowan; Pierre-Henri L Gaillard
Journal:  Cell       Date:  2009-07-10       Impact factor: 41.582

7.  Mammalian BTBD12/SLX4 assembles a Holliday junction resolvase and is required for DNA repair.

Authors:  Jennifer M Svendsen; Agata Smogorzewska; Mathew E Sowa; Brenda C O'Connell; Steven P Gygi; Stephen J Elledge; J Wade Harper
Journal:  Cell       Date:  2009-07-10       Impact factor: 41.582

8.  Bloom's syndrome and EM9 cells in BrdU-containing medium exhibit similarly elevated frequencies of sister chromatid exchange but dissimilar amounts of cellular proliferation and chromosome disruption.

Authors:  J H Ray; J German
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9.  Identification of Holliday junction resolvases from humans and yeast.

Authors:  Stephen C Y Ip; Ulrich Rass; Miguel G Blanco; Helen R Flynn; J Mark Skehel; Stephen C West
Journal:  Nature       Date:  2008-11-20       Impact factor: 49.962

10.  Phosphorylation of Slx4 by Mec1 and Tel1 regulates the single-strand annealing mode of DNA repair in budding yeast.

Authors:  Sonja Flott; Constance Alabert; Geraldine W Toh; Rachel Toth; Neal Sugawara; David G Campbell; James E Haber; Philippe Pasero; John Rouse
Journal:  Mol Cell Biol       Date:  2007-07-16       Impact factor: 4.272

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Review 2.  Control of structure-specific endonucleases to maintain genome stability.

Authors:  Pierre-Marie Dehé; Pierre-Henri L Gaillard
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3.  Dbf4-dependent kinase and the Rtt107 scaffold promote Mus81-Mms4 resolvase activation during mitosis.

Authors:  Lissa N Princz; Philipp Wild; Julia Bittmann; F Javier Aguado; Miguel G Blanco; Joao Matos; Boris Pfander
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4.  An advanced cell cycle tag toolbox reveals principles underlying temporal control of structure-selective nucleases.

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Review 5.  Structure-Specific Endonucleases and the Resolution of Chromosome Underreplication.

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Journal:  Genes (Basel)       Date:  2019-03-19       Impact factor: 4.096

Review 6.  Resolvases, Dissolvases, and Helicases in Homologous Recombination: Clearing the Road for Chromosome Segregation.

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7.  Slx4 and Rtt107 control checkpoint signalling and DNA resection at double-strand breaks.

Authors:  Diego Dibitetto; Matteo Ferrari; Chetan C Rawal; Attila Balint; TaeHyung Kim; Zhaolei Zhang; Marcus B Smolka; Grant W Brown; Federica Marini; Achille Pellicioli
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  7 in total

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